Extracellular vesicles from HTLV-1 infected cells modulate target cells and viral spread

Pinto, Daniel O.; Sharif, Sarah Al; Mensah, Gifty A.; Cowen, Maria; Khatkar, Pooja; Erickson, James; Branscome, Heather; Lattanze, Thomas; DeMarino, Catherine; Alem, Farhang; Magni, R.; Zhou, Weidong; Alais, Sandrine; Dutartre, Hélène; El‐Hage, Nazira; Mahieux, Renaud; Liotta, Lance A.

doi:10.1186/s12977-021-00550-8

Cited by 29 publications

(38 citation statements)

References 114 publications

(112 reference statements)

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“…Lastly, we observed that the HTLV-1infected cells contained higher intracellular env RNA compared to secreted env RNA (EV-bound) at each timepoint (Figure 5A,B). This is consistent with observations that HTLV-1 primarily exists intracellularly, and that infectious virion release occurs sporadically in infected cells [14,18,56,58]. Collectively, these data indicate that HTLV-1 RNA synthesis is increased post-release/induction and that viral RNA can be found in the extracellular environment.…”

Section: Discussionsupporting

confidence: 90%

“…The infectivity of the 24-h samples but not of the 6-h samples could be augmented by the presence of EVs. This is in line with data from Figure 1 (lane 10) that demonstrate that the concentration of EVs peaks at 24 h. Collectively, these results imply that virions released at 24 h are indeed infectious, and the presence of EVs may contribute to their infectivity, since EVs from virally infected cells have been found to contain viral proteins and RNA that can increase the pool of surrounding cells susceptible to infection [14,[18][19][20]32,51,52].…”

Section: Discussionsupporting

confidence: 88%

“…These early EVs contain viral proteins and RNAs that can activate the cell cycle and render naïve recipient T cells and monocytes more vulnerable to subsequent viral infection. Altogether, these data could allow further understanding of the effects of EVs on naïve recipient cells [18,69] and contribute to knowledge about the effects of EVs in enhancing susceptibility to infection. More importantly, these findings show the importance of EVs during viral infection, since they are secreted before the virions and contain several viral proteins with the potential to induce inflammation and disease.…”

Section: Discussionmentioning

confidence: 90%

“…These changes in EV marker expression over time could potentially be due to the increase of EV release at different timepoints (Figure S1). Furthermore, this differential tetraspanin expression could also be attributed to the concept that cells produce different EV populations that are heterogenous in their protein markers [18,30] and that tetraspanins such as CD9 could potentially enhance viral spread and EV biogenesis [45]. Moreover, viral capsid protein p24 was found to interact with CD81 and colocalize in tetraspanin-enriched microdomains composed of CD63, CD9, and CD81, which is crucial for virion assembly [46,47].…”

Section: Discussionmentioning

confidence: 98%

“…EVs carry functional cargoes including viral proteins, lipids, cytokines, RNA and, in some cases, the virion itself (i.e., hepatitis B) [12,13]. As such, EVs are able to modulate disease pathogenesis in several types of infections such as HIV-1, HTLV-1, Ebola virus, and Rift Valley fever by promoting cell-to-cell spread, immune evasion, persistent inflammation, and cell cycle regulation in recipient cells [14][15][16][17][18]. Recently, we found that EVs from HIV-1-infected cells transport TAR RNA to naïve cells, compromising their resistance to HIV-1 through downregulation of apoptosis by depleting CDK9 levels [19].…”

Section: Introductionmentioning

confidence: 99%

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Extracellular Vesicles from Infected Cells Are Released Prior to Virion Release

Kim

Mensah

Sharif

et al. 2021

Cells

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Here, we have attempted to address the timing of EV and virion release from virally infected cells. Uninfected (CEM), HIV-1-infected (J1.1), and human T cell leukemia virus-1 (HTLV-1)-infected (HUT102) cells were synchronized in G0. Viral latency was reversed by increasing gene expression with the addition of serum-rich media and inducers. Supernatants and cell pellets were collected post-induction at different timepoints and assayed for extracellular vesicle (EV) and autophagy markers; and for viral proteins and RNAs. Tetraspanins and autophagy-related proteins were found to be differentially secreted in HIV-1- and HTLV-1-infected cells when compared with uninfected controls. HIV-1 proteins were present at 6 h and their production increased up to 24 h. HTLV-1 proteins peaked at 6 h and plateaued. HIV-1 and HTLV-1 RNA production correlated with viral protein expression. Nanoparticle tracking analysis (NTA) showed increase of EV concentration over time in both uninfected and infected samples. Finally, the HIV-1 supernatant from the 6-h samples was found not to be infectious; however, the virus from the 24-h samples was successfully rescued and infectious. Overall, our data indicate that EV release may occur prior to viral release from infected cells, thereby implicating a potentially significant effect of EVs on uninfected recipient cells prior to subsequent viral infection and spread.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionsupporting

confidence: 88%

Section: Discussionmentioning

confidence: 90%

Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Extracellular Vesicles from Infected Cells Are Released Prior to Virion Release

Kim

Mensah

Sharif

et al. 2021

Cells

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A secretory form of Parkin‐independent mitophagy contributes to the repertoire of extracellular vesicles released into the tumour interstitial fluid in vivo

Howard

Erickson

Cuba

et al. 2022

J of Extracellular Vesicle

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We characterized the in vivo interstitial fluid (IF) content of extracellular vesicles (EVs) using the GFP‐4T1 syngeneic murine cancer model to study EVs in‐transit to the draining lymph node. GFP labelling confirmed the IF EV tumour cell origin. Molecular analysis revealed an abundance of IF EV‐associated proteins specifically involved in mitophagy and secretory autophagy. A set of proteins required for sequential steps of fission‐induced mitophagy preferentially populated the CD81+/PD‐L1+ IF EVs; PINK1, TOM20, and ARIH1 E3 ubiquitin ligase (required for Parkin‐independent mitophagy), DRP1 and FIS1 (mitochondrial peripheral fission), VDAC‐1 (ubiquitination state triggers mitophagy away from apoptosis), VPS35, SEC22b, and Rab33b (vacuolar sorting). Comparing in vivo IF EVs to in vitro EVs revealed 40% concordance, with an elevation of mitophagy proteins in the CD81+ EVs for both murine and human cell lines subjected to metabolic stress. The export of cellular mitochondria proteins to CD81+ EVs was confirmed by density gradient isolation from the bulk EV isolate followed by anti‐CD81 immunoprecipitation, molecular sieve chromatography, and MitoTracker export into CD81+ EVs. We propose the 4T1 in vivo model as a versatile tool to functionally characterize IF EVs. IF EV export of fission mitophagy proteins has broad implications for mitochondrial function and cellular immunology.

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Extracellular vesicle isolation methods identify distinct HIV‐1 particles released from chronically infected T‐cells

Molnar,

Kim,

Wieczorek

et al. 2024

J of Extracellular Vesicle

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The current study analyzed the intersecting biophysical, biochemical, and functional properties of extracellular particles (EPs) with the human immunodeficiency virus type‐1 (HIV‐1) beyond the currently accepted size range for HIV‐1. We isolated five fractions (Frac‐A through Frac‐E) from HIV‐infected cells by sequential differential ultracentrifugation (DUC). All fractions showed a heterogeneous size distribution with median particle sizes greater than 100 nm for Frac‐A through Frac‐D but not for Frac‐E, which contained small EPs with an average size well below 50 nm. Synchronized and released cultures contained large infectious EPs in Frac‐A, with markers of amphisomes and viral components. Additionally, Frac‐E uniquely contained EPs positive for CD63, HSP70, and HIV‐1 proteins. Despite its small average size, Frac‐E contained membrane‐protected viral integrase, detectable only after SDS treatment, indicating that it is enclosed in vesicles. Single particle analysis with dSTORM further supported these findings as CD63, HIV‐1 integrase, and the viral surface envelope (Env) glycoprotein (gp) colocalized on the same Frac‐E particles. Surprisingly, Frac‐E EPs were infectious, and infectivity was significantly reduced by immunodepleting Frac‐E with anti‐CD63, indicating the presence of this protein on the surface of infectious small EPs in Frac‐E. To our knowledge, this is the first time that extracellular vesicle (EV) isolation methods have identified infectious small HIV‐1 particles (smHIV‐1) that are under 50 nm. Collectively, our data indicate that the crossroads between EPs and HIV‐1 potentially extend beyond the currently accepted biophysical properties of HIV‐1, which may have further implications for viral pathogenesis.

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Extracellular vesicles from HTLV-1 infected cells modulate target cells and viral spread

Cited by 29 publications

References 114 publications

Extracellular Vesicles from Infected Cells Are Released Prior to Virion Release

Extracellular Vesicles from Infected Cells Are Released Prior to Virion Release

A secretory form of Parkin‐independent mitophagy contributes to the repertoire of extracellular vesicles released into the tumour interstitial fluid in vivo

Extracellular vesicle isolation methods identify distinct HIV‐1 particles released from chronically infected T‐cells

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